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长期培养的新生胰岛细胞簇在糖尿病逆转方面显示出更好的效果:体内和分子特征。

Long-term cultured neonatal islet cell clusters demonstrate better outcomes for reversal of diabetes: in vivo and molecular profiles.

作者信息

Jimenez-Vera Elvira, Davies Sussan, Phillips Peta, O'Connell Philip J, Hawthorne Wayne J

机构信息

The Centre for Transplant & Renal Research, Westmead Millennium Research Institute, University of Sydney, Westmead, NSW, Australia.

出版信息

Xenotransplantation. 2015 Mar-Apr;22(2):114-23. doi: 10.1111/xen.12151. Epub 2015 Feb 10.

DOI:10.1111/xen.12151
PMID:25676501
Abstract

BACKGROUND

Porcine neonatal islet-like cell clusters (NICC) are being considered as a source of β-cell replacement. However, the lag time to full function due to hormonal immaturity remains a problem. This study aimed to determine whether time in culture was important for NICC function in vivo.

METHODS

Neonatal islet-like cell clusters were isolated from piglets aged between 1 and 3 days, and cultured for up to 27 days post-isolation. Each week, NICC number, viability, and function were determined.

RESULTS

Neonatal islet-like cell clusters cultured for 12, 19, and 27 days achieved normal blood glucose levels at 46 days (85% of animals), 32 days (100% of animals), and 35 days (81% of animals), respectively. By comparison, standard 6-day culture took a mean of 63 days to achieve normoglycemia in 35% of animals. Longer time in culture resulted in a significant loss of islet equivalent over time. However, insulin gene expression levels were significantly higher at days 12, 19, 27 compared to day 6. Glucagon gene expression was highest at day 12, and significantly higher than day 6 at all time points. Bcl-2 gene expression increased over time, and tissue factor (TF) gene expression was highest on day 6 and then decreased over the remaining time points.

CONCLUSION

Culture of NICC for 12 days provides the best balance in vivo functional outcome for transplantation, shown by better reversal of diabetes, and higher levels of gene expression for insulin, glucagon and Bcl-2 and lower levels of TF expression with acceptable NICC number loss in terms of time and expense.

摘要

背景

猪新生儿胰岛样细胞簇(NICC)被视为β细胞替代的一个来源。然而,由于激素不成熟导致的完全发挥功能的延迟时间仍然是一个问题。本研究旨在确定培养时间对NICC体内功能是否重要。

方法

从1至3日龄仔猪分离出新生儿胰岛样细胞簇,并在分离后培养长达27天。每周测定NICC数量、活力和功能。

结果

培养12天、19天和27天的新生儿胰岛样细胞簇分别在46天(85%的动物)、32天(100%的动物)和35天(81%的动物)达到正常血糖水平。相比之下,标准的6天培养平均需要63天才能使35%的动物实现血糖正常。随着培养时间延长,胰岛当量随时间显著减少。然而,与第6天相比,第12天、19天、27天的胰岛素基因表达水平显著更高。胰高血糖素基因表达在第12天最高,且在所有时间点均显著高于第6天。Bcl-2基因表达随时间增加,组织因子(TF)基因表达在第6天最高,然后在其余时间点下降。

结论

培养12天的NICC在移植的体内功能结果方面提供了最佳平衡,表现为糖尿病逆转更好,胰岛素、胰高血糖素和Bcl-2的基因表达水平更高,TF表达水平更低,且在时间和费用方面NICC数量损失可接受。

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